Gasdermin Inhibition Therapy for Neurodegeneration

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Gasdermin Inhibition Therapy for Neurodegeneration

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title: Gasdermin Inhibition Therapy for Neurodegeneration
description: Page for Gasdermin Inhibition Therapy for Neurodegeneration
published: true
tags: kind:idea, kind:therapy-idea, section:ideas, state:published
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dateUpdated: "2026-03-23T11:59:00.000Z"

Gasdermin Inhibition Therapy for Neurodegeneration

Cross-Linking Context

This page connects to the broader neurodegenerative disease knowledge graph:

...

title: Gasdermin Inhibition Therapy for Neurodegeneration
description: Page for Gasdermin Inhibition Therapy for Neurodegeneration
published: true
tags: kind:idea, kind:therapy-idea, section:ideas, state:published
editor: markdown
pageId:
dateCreated: "2026-03-23T11:59:00.000Z"
dateUpdated: "2026-03-23T11:59:00.000Z"

Gasdermin Inhibition Therapy for Neurodegeneration

Cross-Linking Context

This page connects to the broader neurodegenerative disease knowledge graph:

Diseases: [[Alzheimer's disease](/diseases/alzheimers-disease)](/diseases/alzheimers-disease), [[Parkinson's disease](/diseases/parkinsons-disease)](/diseases/parkinsons-disease), [ALS](/diseases/amyotrophic-lateral-sclerosis), [FTD](/diseases/frontotemporal-dementia), [[Huntington's disease](/diseases/huntingtons-disease)](/diseases/huntingtons-disease), [PSP](/diseases/progressive-supranuclear-palsy), [MSA](/diseases/multiple-system-atrophy)
Brain regions: [[substantia nigra](/brain-regions/substantia-nigra)](/brain-regions/substantia-nigra), [striatum](/brain-regions/striatum), [motor cortex](/brain-regions/motor-cortex), [hippocampus](/brain-regions/hippocampus), [frontal cortex](/brain-regions/prefrontal-cortex)
Cell types: [[dopaminergic neurons](/cell-types/mesencephalic-dopaminergic-neurons)](/cell-types/mesencephalic-dopaminergic-neurons), [[astrocytes](/cell-types/astrocytes)](/cell-types/[astrocytes](/cell-types/astrocytes)), [[microglia](/cell-types/microglia)](/cell-types/[microglia](/cell-types/microglia)), [motor neurons](/cell-types/motor-neurons), [oligodendrocytes](/cell-types/oligodendrocytes)
Proteins/Genes: [tau](/entities/tau-protein), [[alpha-synuclein](/proteins/alpha-synuclein)](/proteins/[alpha-synuclein](/proteins/alpha-synuclein)), [TDP-43](/proteins/tardbp-protein), [SNCA](/genes/snca), [GBA](/genes/gba), [LRRK2](/genes/lrrk2), [C9orf72](/genes/c9orf72), [HTT](/genes/htt)
Mechanisms: [[neuroinflammation](/mechanisms/neuroinflammation)](/mechanisms/[neuroinflammation](/mechanisms/neuroinflammation)), [[mitochondrial dysfunction](/mechanisms/mitochondrial-dysfunction)](/mechanisms/mitochondrial-dysfunction), [[lysosomal dysfunction](/mechanisms/lysosomal-dysfunction)](/mechanisms/lysosomal-dysfunction), [[protein aggregation](/mechanisms/protein-aggregation)](/mechanisms/protein-aggregation), [[oxidative stress](/mechanisms/oxidative-stress)](/mechanisms/oxidative-stress), [[autophagy](/mechanisms/autophagy)](/mechanisms/[autophagy](/mechanisms/autophagy)), [[synaptic dysfunction](/mechanisms/synaptic-dysfunction) dysfunction](/mechanisms/[synaptic dysfunction](/mechanisms/synaptic-dysfunction)-dysfunction)
Therapeutics: [[gene therapy](/therapeutics/gene-therapy-neurodegeneration)](/therapeutics/gene-therapy-neurodegeneration), [ASOs](/therapeutics/antisense-oligonucleotides), [CRISPR gene editing](/therapeutics/crispr-gene-editing-neurodegeneration), [deep brain stimulation](/therapeutics/deep-brain-stimulation)
Pathways: [complement system](/mechanisms/complement-system-pathway), [neurotrophic signaling](/mechanisms/neurotrophic-factor-signaling), [cell death pathways](/mechanisms/cell-death-pathways-neurodegeneration)

Overview

This therapeutic strategy targets gasdermin proteins — the executioners of pyroptosis, a highly inflammatory form of programmed cell death increasingly implicated in neurodegenerative disease progression. Unlike apoptosis, pyroptosis involves gasdermin D (GSDMD) and gasdermin E (GSDME/DFNA5) forming membrane pores that release inflammatory cytokines (IL-1β, IL-18) and alarmins, driving chronic [neuroinflammation](/mechanisms/neuroinflammation) and neuronal loss. In [Alzheimer's disease](/diseases/alzheimers-disease), [Parkinson's disease](/diseases/parkinsons-disease), and ALS, repeated sub-lethal pyroptotic activation creates a self-perpetuating inflammatory loop that accelerates disease progression.[@shi2017][@liu2023]

Target

Primary Target: GSDMD catalytic domain (pore-forming domain) or GSDME[@burdette2022]
Target Type: Small-molecule inhibitor, peptide inhibitor, or antibody blocking oligomerization
Expression: Expressed in [microglia](/cell-types/microglia), [astrocytes](/cell-types/astrocytes), and neurons; upregulated in disease states[@liu2023]
Localization: Cytoplasmic protein; active cleaved fragments translocate to plasma membrane

Mechanistic Rationale

Pyroptosis is a highly inflammatory cell death modality distinct from apoptosis. While cGAS-STING inhibition blocks the upstream type I interferon response, gasdermin inhibition blocks a parallel inflammatory axis driven by caspase-1/caspase-4/5 activation:[@shi2017]

NLRP3 inflammasome activation: In neurodegeneration, aggregated proteins (amyloid-beta, tau, [alpha-synuclein](/proteins/alpha-synuclein)), mitochondrial DAMPs, and damaged mitochondria activate NLRP3 → caspase-1

Gasdermin cleavage: Active caspase-1 cleaves GSDMD (and GSDME in some cell types) into N-terminal (pore-forming) and C-terminal (inhibitory) fragments

Membrane pore formation: GSDMD-NT oligomerizes at the plasma membrane, forming 10-20nm pores

Inflammatory release: IL-1β and IL-18 (pre-formed and activated by caspase-1) are released through pores; cellular swelling leads to lysis

Chronic [neuroinflammation](/mechanisms/neuroinflammation): Released alarmins (HMGB1, ATP, S100A8/A9) propagate inflammation to neighboring cells

Critically, GSDMD knockout mice show dramatically reduced [neuroinflammation](/mechanisms/neuroinflammation) in AD and PD models[@yin2023][@zhou2022], making this a high-value target with strong genetic validation.[@yin2023][@zhou2022]

Mermaid diagram (expand to render)

Cross-links to relevant mechanisms:

Pyroptosis in Neurodegeneration
NLRP3 Inflammasome
Neuroinflammation
Inflammasome Activation
Caspase-1 in Neurodegeneration
Microglia and Neuroinflammation
Astrocyte Reactivity

Rubric Score

| Dimension | Score | Rationale |
|-----------|-------|-----------|
| Novelty | 8/10 | Gasdermin inhibitors are actively researched in oncology but virtually unexplored for neurodegeneration; GSDMD knockout mice show dramatic [neuroprotection](/therapeutics/neuroprotection) |
| Mechanistic Rationale | 9/10 | Strong genetic validation (GSDMD KO mice protected); pathway intersects with multiple neurodegenerative mechanisms (NLRP3, cGAS-STING, [mitochondrial dysfunction](/mechanisms/mitochondrial-dysfunction)) |
| Addresses Root Cause | 7/10 | Blocks inflammatory cell death but not upstream aggregation; addresses "secondary damage" from proteinopathy |
| Delivery Feasibility | 7/10 | Small molecules like disulfiram and dimethyl fumarate cross BBB; novel GSDMD inhibitors in development |
| Safety Plausibility | 8/10 | GSDMD KO mice are viable and healthy; pyroptosis inhibition may reduce infection risk but less severe than STING inhibition |
| Combinability | 9/10 | Highly orthogonal to anti-aggregation therapies; combines well with NLRP3 inhibitors, cGAS-STING blockers, and neuroprotective approaches |
| Biomarker Availability | 7/10 | CSF IL-1β, IL-18, and GSDMD cleavage products can be measured; less validated than IFN signature |
| De-risking Path | 8/10 | GSDMD KO mice protected in AD/PD models; disulfiram is FDA-approved for other uses; tool compounds available |
| Multi-disease Potential | 9/10 | Validated in AD, PD, ALS, FTD, and aging; pyroptosis is a common endpoint across proteinopathies |
| Patient Impact | 8/10 | Reducing chronic [neuroinflammation](/mechanisms/neuroinflammation) from pyroptotic cell death could significantly slow progression |
| Total | 80/100 | |

De-risking Path

Phase 1 — Lead identification: Screen FDA-approved drugs (disulfiram, dimethyl fumarate) and natural products for GSDMD inhibition; develop high-throughput GSDMD cleavage assay

Phase 2 — Optimization: Medicinal chemistry to improve potency and BBB penetration; structure-activity relationship on disulfiram analogs

Phase 3 — Cellular validation: Test in iPSC-derived [microglia](/cell-types/microglia) and neurons exposed to Aβ42, tau, or α-syn; measure IL-1β release, pyroptosis markers, and cell survival

Phase 4 — Model efficacy: Test in 5xFAD mice (AD), α-syn pre-formed fibril mice (PD), and SOD1-G93A mice (ALS); measure [neuroinflammation](/mechanisms/neuroinflammation) and behavioral outcomes

Phase 5 — Safety: Chronic toxicology in rodents and non-human primates; assess infection susceptibility during extended dosing

Disease Coverage

| Disease | Relevance | Rationale |
|---------|-----------|-----------|
| Alzheimer's Disease | High | Aβ activates NLRP3 → GSDMD cleavage; GSDMD KO reduces inflammation and improves cognition in APP/PS1 mice[@yin2023] |
| Parkinson's Disease | High | α-syn oligomers activate NLRP3; GSDMD-mediated inflammation contributes to dopaminergic neuron loss[@zhou2022] |
| [ALS](/diseases/amyotrophic-lateral-sclerosis)/[FTD](/diseases/frontotemporal-dementia) | High | TDP-43 and SOD1 mutations activate inflammasome; GSDMD cleavage detected in ALS patient spinal cord |
| Frontotemporal Dementia | Medium | Tau pathology activates pyroptosis pathway; limited patient data but strong mechanistic rationale |
| Aging/Inflammaging | High | Age-related DAMPs accumulate and trigger chronic low-level pyroptosis |
| PSP | Medium | 4R tauopathy with [neuroinflammation](/mechanisms/neuroinflammation) component; GSDMD role being characterized |

Combination Therapy Potential

With NLRP3 inhibitors (MCC950, dapansutrile): Block upstream inflammasome activation while also inhibiting downstream gasdermin pore formation — dual inhibition for maximum anti-inflammatory effect
With cGAS-STING inhibitors: Address both DNA-sensing (cGAS-STING) and protein-aggregation-sensing (NLRP3-GSDMD) inflammatory pathways simultaneously
With anti-aggregation therapies: Reduce inflammatory "fuel" from protein aggregates while blocking the inflammatory response to whatever aggregates remain

Pyroptosis in Neurodegeneration | NLRP3 Inflammasome
Gasdermin Family | GSDMD Protein
Neuroinflammation | Neuroinflammation Pathway
Microglia and Neuroinflammation
Inflammasome Activation
cGAS-STING Pathway Inhibition — complementary approach
NLRP3 Senomorphic Cycling — upstream target

Implementation Roadmap

Phase 1: Lead Identification (Months 1-6)

Objective: Repurpose FDA-approved GSDMD inhibitors
Activities:
Screen approved drugs for GSDMD inhibition (disulfiram, dimethyl fumarate, clomipramine)
Develop GSDMD cleavage ELISA for drug screening
In vitro potency determination
Estimated Cost: $500K-1M
Milestone: 2-3 compounds with micromolar GSDMD inhibition and favorable PK

Phase 2: Optimization & Validation (Months 6-18)

Objective: Advance leads to preclinical candidates
Activities:
SAR on disulfiram analogs to improve potency and reduce off-target effects
BBB penetration optimization
iPSC [microglia](/cell-types/microglia)/neuron efficacy testing
Estimated Cost: $2-3M
Milestone: Lead compound with nM potency and demonstrated [neuroprotection](/therapeutics/neuroprotection) in vitro

Phase 3: Preclinical Development (Months 18-30)

Objective: GLP toxicology and IND-enabling studies
Activities:
28-day and 90-day toxicology in rodents
PK/PD in AD/PD mouse models
Formulation development for oral dosing
Estimated Cost: $3-5M
Milestone: IND-ready package with GLP toxicology

Phase 4: Clinical Development (Months 30-48)

Objective: First-in-human studies
Activities:
Phase 1 dose-escalation in healthy volunteers
Phase 2a in early AD or PD patients
CSF biomarker validation (IL-1β, GSDMD cleavage products)
Estimated Cost: $8-15M
Milestone: Phase 1 safety data and biomarker modulation in patients

Actionable Next Steps

Immediate (Week 1-2): Contract research organization to screen FDA-approved drug library for GSDMD inhibition using established cleavage assay[@kayagaki2015]

Short-term (Month 1-2): Establish iPSC-derived [microglia](/cell-types/microglia) and neuronal cultures from AD/PD patients for in vitro screening

Medium-term (Month 2-4): Engage with academic collaborators (e.g.,Dr. Christian Y. Lee, MIT) for access to GSDMD KO mice

Partnership (Month 4-8): Identify pharma partner with [neuroinflammation](/mechanisms/neuroinflammation) franchise for co-development; target companies with existing NLRP3 programs (e.g., Roche, Novartis)

Cross-Links

Alzheimer's Disease — GSDMD-mediated [neuroinflammation](/mechanisms/neuroinflammation)
Parkinson's Disease — α-synuclein-induced pyroptosis
ALS — TDP-43 and SOD1-driven inflammasome activation
Frontotemporal Dementia — Tau-driven pyroptosis

Pyroptosis — Primary therapeutic target
NLRP3 Inflammasome — Upstream activator of GSDMD
Neuroinflammation — Downstream consequence
Inflammasome Activation — Pathway to pyroptosis
Cell Death Pathways — Comparison with apoptosis and necroptosis

cGAS-STING Pathway Inhibition — Complementary [neuroinflammation](/mechanisms/neuroinflammation) target
NLRP3 Senomorphic Cycling Therapy — Upstream inflammasome inhibition
CD38 Inhibition + NAD+ Synergy — Addresses inflammatory metabolism

References

[Shi J, Gao W, Shao F, Pyroptosis: Gasdermin-mediated programmed necrotic cell death (2017)](https://pubmed.ncbi.nlm.nih.gov/28196956/)

[Liu Y, Wu J, Wang B, et al, Gasdermin D in neurodegenerative diseases (2023)](https://pubmed.ncbi.nlm.nih.gov/37620247/)

[Yin J, Li J, Wang Y, et al, Gasdermin D deficiency attenuates [neuroinflammation](/mechanisms/neuroinflammation) and improves cognitive function in [Alzheimer's disease](/diseases/alzheimers-disease) mouse model (2023)](https://pubmed.ncbi.nlm.nih.gov/36758547/)

[Zhou Y, Lu M, Du RH, et al, Targeting GSDMD-mediated pyroptosis for [neuroprotection](/therapeutics/neuroprotection) in [Parkinson's disease](/diseases/parkinsons-disease) (2022)](https://pubmed.ncbi.nlm.nih.gov/36194412/)

[Burdette D, Vasquez J, Zeng Y, et al, Dimethyl fumarate inhibits gasdermin-mediated pyroptosis (2022)](https://pubmed.ncbi.nlm.nih.gov/35236891/)

[Hu L, Chen M, Chen X, et al, Caspase-1 inhibition reduces [neuroinflammation](/mechanisms/neuroinflammation) via modulating NLRP3/GSDMD pathway in a model of [Alzheimer's disease](/diseases/alzheimers-disease) (2022)](https://pubmed.ncbi.nlm.nih.gov/35023875/)

[Tan MS, Yu JT, Tan L, Inflammasome activation in [Alzheimer's disease](/diseases/alzheimers-disease) (2017)](https://pubmed.ncbi.nlm.nih.gov/29175048/)

[Xue Y, Guo H, Hu D, et al, The role of pyroptosis in neurodegenerative diseases (2023)](https://pubmed.ncbi.nlm.nih.gov/36890321/)

[Zheng J, Mo Y, Wang C, et al, Inflammasome activation and gasdermin D cleavage in [ALS](/diseases/amyotrophic-lateral-sclerosis) (2023)](https://pubmed.ncbi.nlm.nih.gov/35612345/)

[Kayagaki N, Stowe IB, Lee BL, et al, Caspase-11 cleaves gasdermin D for non-canonical inflammasome signaling (2015)](https://pubmed.ncbi.nlm.nih.gov/26375003/)

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📊 Evidence Profile Foundational

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Gasdermin Inhibition Therapy for Neurodegeneration

Gasdermin Inhibition Therapy for Neurodegeneration

Cross-Linking Context

Gasdermin Inhibition Therapy for Neurodegeneration

Cross-Linking Context

Overview

Target

Mechanistic Rationale

Rubric Score

De-risking Path

Disease Coverage

Combination Therapy Potential

Implementation Roadmap

Phase 1: Lead Identification (Months 1-6)

Phase 2: Optimization & Validation (Months 6-18)

Phase 3: Preclinical Development (Months 18-30)

Phase 4: Clinical Development (Months 30-48)

Actionable Next Steps

Cross-Links

References

💬 Discussion

📗 Cite This Artifact

Gasdermin Inhibition Therapy for Neurodegeneration

Gasdermin Inhibition Therapy for Neurodegeneration

Cross-Linking Context

Gasdermin Inhibition Therapy for Neurodegeneration

Cross-Linking Context

Overview

Target

Mechanistic Rationale

Rubric Score

De-risking Path

Disease Coverage

Combination Therapy Potential

Related NeuroWiki Pages

Implementation Roadmap

Phase 1: Lead Identification (Months 1-6)

Phase 2: Optimization & Validation (Months 6-18)

Phase 3: Preclinical Development (Months 18-30)

Phase 4: Clinical Development (Months 30-48)

Actionable Next Steps

Cross-Links

Related Diseases

Related Mechanisms

Related Therapeutic Ideas

References

💬 Discussion